| Literature DB >> 26252880 |
Yongmei Yang1, Ailin Qu1, Jingkang Liu1, Rui Wang1, Yingjie Liu1, Gang Li2, Weili Duan1, Qian Fang1, Xiumei Jiang1, Lili Wang1, Guixi Zheng1, Lutao Du1, Xin Zhang1, Chuanxin Wang1.
Abstract
MiR-210 is the master hypoxamir that generally exhibits oncogenic properties in most human solid tumors including bladder cancer (BC). However, it remains unknown about the clinical significance of circulating miR-210 levels in BC. In this study, we found that serum miR-210 was up-regulated in patients with BC, and serum levels of miR-210 increased with advancing stage and grade. Moreover, serum miR-210 expression was found to be significantly reduced in paired post-operative samples and elevated in most patients with relapsed BC. Taken together, our data suggest that serum miR-210 could be a potential noninvasive biomarker for screening, predicting and monitoring BC.Entities:
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Year: 2015 PMID: 26252880 PMCID: PMC4529273 DOI: 10.1371/journal.pone.0135168
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Fig 1The miR-210 expression in primary BC tissues and BC cell lines.
(A) Comparison of miR-210 levels in 40 pairs of primary BC tissues and adjacent normal tissues. The expression level of miR-210 was significant higher in primary BC tissues than in adjacent normal tissues (P<0.001). (B) The expression levels of miR-210 in BC cell lines were higher than in a human uroepithelial cell line.
Fig 2(A) The serum miR-210 expression in 168 BC patients and 104 controls. The upper and lower limits of the boxes and the lines inside the boxes indicate the 75th and 25th percentiles and the median, respectively. The upper and lower horizontal bars denote the 90th and 10th percentiles, respectively. (B) Receiver-operating characteristic (ROC) curve analysis of the serum miR-210 to detect BC patients. The AUC of 0.898 (95% CI 0.855–0.931) indicates good discriminative power.
MiR-210 expression and clinicaopathological feature in BC patients [median (interquartile range)].
| Clinicopathological feature | NO. of cases | miR-210 expression |
|
|---|---|---|---|
| Gender | 0.475 | ||
| Male | 128 | 58.680 (39.110–72.473) | |
| Female | 40 | 54.360 (31.440–89.780) | |
| Age | 0.438 | ||
| Under 65 | 74 | 57.260 (39.350–74.128) | |
| 65 or more | 94 | 56.990 (37.043–72.263) | |
| Grade | 0.058 | ||
| G1 | 48 | 50.620 (31.513–69.203) | |
| G2 | 50 | 54.785 (37.048–69.523) | |
| G3 | 70 | 61.890 (42.170–76.770) | |
| T stage | 0.000 | ||
| Ta–T1 | 84 | 45.805(30.023–60.478) | |
| T2–T4 | 84 | 69.025 (54.336–85.915) | |
| N stage | 0.081 | ||
| N0 | 146 | 56.435 (38.378–69.780) | |
| N1-3 | 22 | 72.315 (37.613–116.763) | |
| M stage | 0.040 | ||
| M0 | 154 | 56.285 (38.298–71.558) | |
| M1-3 | 14 | 71.390 (58.233–88.020) |
aStatistical significance was determined by the Kruskal-Wallis test.
bStatistical significance was determined by the Mann-Whitey U test.
c The mean age of the patients is 64.8.
Fig 3(A) The serum miR-210 expression in 84 NMIBC, 84 MIBC and 104 controls. All P<0.05/3. (B) ROC curves for serum miR-210 for NMIBC group (n = 84) vs healthy individuals (n = 104). AUC = 0.858 (95% CI 0.800–0.904). (C) ROC curves for serum miR-210 for MIBC group (n = 84) vs healthy individuals (n = 104). AUC = 0.938 (95% CI 0.893–0.968). (D) ROC curves for serum miR-210 for NMIBC group (n = 84) vs MIBC group (n = 84). AUC = 0.736 (95% CI 0.662–0.800).
Fig 4Comparison of circulating miR-210 expressions in different groups.
(A) Comparison of serum miR-210 expressions between pre- and post-operative samples from BC patients. The serum miR-210 levels were significantly reduced in paired post-operative samples compared with those in pre-operative samples (P<0.0001). (B) Scatter plot of miR-210 levels in the pre-operative (n = 168), post-operative (n = 40) and relapse (n = 30) serum groups.
Fig 5Comparison of medium miR-210 level in BC cells (5637 and T24).
Increased tendencies were confirmed in cell medium in both cell number- and time-course-dependent manners.